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首页> 外文期刊>Cancer genomics & proteomics >Expression of Signal-induced Proliferation-associated Gene 1 (SIPA1), a RapGTPase-activating Protein, Is Increased in Colorectal Cancer and Has Diverse Effects on Functions of Colorectal Cancer Cells
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Expression of Signal-induced Proliferation-associated Gene 1 (SIPA1), a RapGTPase-activating Protein, Is Increased in Colorectal Cancer and Has Diverse Effects on Functions of Colorectal Cancer Cells

机译:RapGTPase激活信号,信号诱导的增殖相关基因1(SIPA1)的表达在结直肠癌中增加,并且对结直肠癌细胞的功能具有不同的影响

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Background: Signal-induced proliferation-associated gene 1 (SIPA1) codes for a GTPase-activating protein, known to be a negative regulator of Ras-related Protein (RAP) which belongs to the Ras superfamily. It has been implicated in certain malignancies, including leukemia, cervical cancer and breast cancer. However the role of this molecule in colorectal cancer remains unknown. The current study aimed to investigate the expression of SIPA1 in colorectal tumour tissues and its impact on the function of colorectal cancer cells. Materials and Methods: A total of 94 colorectal cancer tissues together with 80 normal background tissues were used to examine the expression of SIPA1 transcript and protein using real-time quantitative Polymerase Chain Reaction (PCR) and immunohistochemical methods, respectively. Any association with clinical and histopathological characteristics was then identified. Ribozyme transgenes targeting SIPA1 were prepared to knockdown the expression of SIPA1 in colorectal cancer cells. The impact on their functions was subsequently determined, using respective in vitro function assays. Results: An increased expression of SIPA1 was evident in colorectal cancer tissues compared with its expression in normal background tissues (p<0.001). In colorectal tumours, its expression appeared to be lower in poorly-differentiated samples and in patients who had lymphatic metastasis. Knockdown of SIPA1 in colorectal cancer cells resulted in reduced cell growth in vitro. The knockdown exhibited a contrasting effect on invasion and migration, both of which were increased in SIPA1-knockdown cells compared with the controls. Conclusion: SIPA1 is up-regulated in colorectal cancer. This suggests that SIPA1 plays diverse roles during disease progression as has contrasting effects on growth and motility of colorectal cancer cells.
机译:背景:信号诱导的增殖相关基因1(SIPA1)编码GTPase激活蛋白,该蛋白是Ras相关蛋白(RAP)的负调控因子,RAP相关蛋白属于Ras超家族。它与某些恶性肿瘤有关,包括白血病,宫颈癌和乳腺癌。然而,该分子在结直肠癌中的作用仍然未知。当前的研究旨在研究SIPA1在大肠肿瘤组织中的表达及其对大肠癌细胞功能的影响。材料与方法:总共94个结直肠癌组织和80个正常背景组织分别通过实时定量聚合酶链反应(PCR)和免疫组织化学方法检测了SIPA1转录本和蛋白质的表达。然后确定与临床和组织病理学特征的任何关联。制备靶向SIPA1的核酶转基因以敲低SIPA1在大肠癌细胞中的表达。随后使用各自的体外功能测定法确定对其功能的影响。结果:与正常背景组织中的表达相比,SIPA1在大肠癌组织中的表达明显增加(p <0.001)。在大肠肿瘤中,其表达在低分化样品和淋巴结转移患者中似乎较低。在大肠癌细胞中抑制SIPA1导致体外细胞生长减少。击倒表现出对侵袭和迁移的对比作用,与对照相比,在SIPA1击倒细胞中两者均增加。结论:SIPA1在结直肠癌中表达上调。这表明SIPA1在疾病进展过程中扮演着各种角色,对结直肠癌细胞的生长和运动具有相反的影响。

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